Blood Concentrations of Homocysteine and Methylmalonic Acid among Demented and Non-Demented Swedish Elderly with and without Home Care Services and Vitamin B(12) Prescriptions

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Hagnelius, N., Wahlund, L., Schneede, J., Nilsson, T. (2012)

Blood Concentrations of Homocysteine and Methylmalonic Acid among Demented and Non-Demented Swedish Elderly with and without Home Care Services and Vitamin B(12) Prescriptions.

Dementia and geriatric cognitive disorders extra, 2(1): 387-99 http://dx.doi.org/10.1159/000339669

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Original Research Article

Blood Concentrations of Homocysteine and Methylmalonic Acid among

Demented and Non-Demented Swedish Elderly with and without Home Care Services and Vitamin B ₁₂ Prescriptions

Nils-Olof Hagnelius

Lars-Olof Wahlund

Jörn Schneede

Torbjörn K. Nilsson

a Department of Geriatric Medicine, Örebro University Hospital, School of Health and Medical Sciences, Örebro University, and ^b Department of Laboratory Medicine, Division of Clinical Chemistry, Örebro University Hospital, Örebro , ^c Department of Neurobiology, Care Sciences and Society, Section of Clinical Geriatrics, Karolinska Institutet, Stockholm , and ^d Department of Pharmacology and Clinical Neuroscience, Division of Clinical Pharmacology, University Hospital of Northern Sweden, Umeå , Sweden

Key Words

Homocysteine ⴢ Dementia ⴢ Vitamin B 12 ⴢ Folate ⴢ Home care service

Abstract

Background and Aims: Total plasma homocysteine (tHcy) has been suggested as a risk factor of dementia. Our aim was to investigate potential differences in tHcy status in relation to the prescription of vitamin B ₁₂ and dementia diagnosis. We examined whether vitamin B ₁₂ prescrip- tions, a family history of dementia, or the need for home care service might be associated with tHcy values. Methods: A cross-sectional monocenter study comprising 926 consecutive sub- jects attending our Memory Care Unit was conducted. Results: Demented subjects being pre- scribed vitamin B ₁₂ had higher serum vitamin B ₁₂ (p = 0.025) but also higher tHcy (p ! 0.001) and serum methylmalonate (p = 0.032), and lower serum folate (p ! 0.001) than those who did not receive vitamin B ₁₂ prescriptions. tHcy levels were significantly higher in non-demented sub- jects receiving home care service (p = 0.007). This group also had lower serum albumin (demen- tia: p ! 0.001; non-dementia: p = 0.004). There was no difference in renal function (estimated glomerular filtration rate) in demented or non-demented subjects with or without vitamin B ₁₂ prescriptions (dementia with/without vitamin B ₁₂ prescription: p = 0.561; non-dementia with/

Nils-Olof Hagnelius

NonCommercial-NoDerivs 3.0 License (www.karger.com/OA-license), applicable to the online version of the article only. Distribution for non-commercial purposes only.

Department of Geriatric Medicine Örebro University Hospital SE–701 85 Örebro (Sweden)

Tel. +46 19 602 1000, E-Mail nils-olof.hagnelius @ orebroll.se

Demented and Non-Demented Swedish Elderly

without vitamin B ₁₂ prescription: p = 0.710). Conclusion: Despite vitamin B ₁₂ prescriptions, de- mented subjects had higher tHcy and methylmalonate values. The elevated metabolite values could not be explained by differences in renal function. Thus, elderly subjects on vitamin B ₁₂ prescription appear to have unmet nutritional needs. Copyright © 2012 S. Karger AG, Basel

Introduction

There has been a growing interest in the role of vitamin deficiencies in relation to de- mentia. Vitamin B ₁₂ was among the first vitamins being investigated in relation to neuropsy- chiatric disease, and already in the mid-19th century, Addison [1] described neuropsychiat- ric symptoms in patients with pernicious anemia (‘the mind occasionally wanders’). There are reports on improvement of mental symptoms upon vitamin B 12 supplementation [2, 3] . In addition to insufficient vitamin B ₁₂ status, folate deficiency has also been discussed in the pathogenesis of dementia [4–8] . A prospective Canadian study among older persons found that low serum folate was associated with a higher risk of cerebrovascular events including vascular dementia and death because of stroke [9] .

The essential amino acid methionine, together with vitamin B ₁₂ and folate, is centrally involved in the one-carbon metabolism. Methionine serves in its activated form, S-adenosyl- methionine (SAM), as the principal one-carbon donor in the body. In the course of methyl group transfer from SAM, homocysteine (Hcy) is formed. Total plasma Hcy (tHcy) has been suggested as an independent risk factor for dementia and Alzheimer’s disease [10–12] . There are a number of significant predictors of tHcy, such as serum folate [13] , serum vitamin B ₁₂ [14] and serum creatinine [15] , but it is debated whether elevated tHcy is only a marker of or causally involved in the pathogenesis of cardiovascular disease and dementias [16] .

A family history of dementia approximately doubles the lifetime risk of developing de- mentia [17] . Although the exact mechanisms are unknown, genetic, nutritional and environ- mental factors might contribute to the associations between dementia and tHcy, as many of these factors are common risk factors for both dementia and hyperhomocysteinemia. Thus, tHcy-related variables should also be studied in relation to family history of dementia.

Home care service (HCS) is intended to care for older people with and without dementia, to help them manage their own homes and to prevent premature institutionalization. As HCS in the majority of cases includes prefabricated food service (‘meals on wheels’), it is of great importance to investigate how this food service influences nutrition in general and tHcy-related micronutrients in particular. Unfortunately, little attention has been paid to the risk of quantitative and qualitative malnutrition in the elderly [18] . However, the clinical util- ity of tHcy and its determinants in the laboratory work-up of patients with suspected demen- tia, as an adjunct to traditional patient history and demographic variables [19–21] , is far from clear, and integrative studies in an out-patient based setting are required.

At the Memory Care Unit of the Department of Geriatrics, Örebro University Hospital, Sweden, a database was established in the mid-1990s to keep track of the patient records and to monitor the quality of the medical service concerning cognitive disorders. In the present study, we used this database to evaluate different patient history and demographic variables, as well as selected serum biomarkers as predictors of dementia in a consecutive series of 926 persons. The aim of the present study was to investigate potential differences in tHcy and its determinants [serum vitamin B 12 , serum folate, serum creatinine and estimated glomerular filtration rate (eGFR)] in relation to the diagnosis of dementia. We also wanted to investigate associations between tHcy and vitamin B 12 prescriptions, a family history of dementia as well as HCS requirements.

Demented and Non-Demented Swedish Elderly

Materials and Methods

Study Population

A database for monitoring the efficacy of various diagnostic markers and patient history data for differentiating between clinical dementia and non-dementia conditions in our Mem- ory Care Unit was established in late 1995. The database comprises 926 consecutive subjects (366 men and 560 women) referred to the Memory Care Unit at the Geriatric Department, Örebro Medical Center Hospital, Örebro, Sweden, between 1996 and 2000 for diagnostic evaluation of suspected cognitive impairment. In this monocenter cross-sectional study, three specialists in geriatric medicine with comprehensive training in cognitive medicine per- formed a clinical investigation of these subjects. Dementia was diagnosed according to DSM- III-R criteria [22] , which included medical history, physical examination, together with neu- rological, psychiatric and neuropsychological examination, and laboratory tests. At the time of patient recruitment, there was still no widespread use of multi-B vitamin supplements con- taining pharmacological vitamin B ₁₂ doses (0.5 mg/tablet) through doctor’s prescription in Sweden, whereas around 15% of subjects aged 6 70 years were on high-dose oral (1 mg/day) or parenteral vitamin B ₁₂ treatment and approximately 3% were on folic acid treatment [23] .

A wide range of biochemical blood tests and patient history variables was entered into the database. In the present study, we focus on the following variables: prescription of high- dose oral or intermittent parenteral vitamin B 12 preparations (yes/no), family history of de- mentia (yes/no) and the use of HCS (yes/no). The data on vitamin B ₁₂ prescriptions was based on patient and caregiver history and refers only to high-dose oral (1-mg vitamin B ₁₂ tablets) or parenteral preparations (1 mg/ml). The dosage interval of parenteral vitamin B 12 doses varied from 1 mg once a month to 1 mg every third month. High-dose oral treatment ac- counted for approximately 70% of vitamin B 12 prescriptions. In addition, we included the results from the Mini Mental State Examination (MMSE) tests in the analysis. Furthermore, data of serum biomarkers obtained by clinical routine testing at the time of recruitment [e.g.

blood hemoglobin (B-Hb), blood mean cellular volume (B-MCV), serum albumin, plasma creatinine, serum folate, serum vitamin B 12 , plasma tHcy, serum methylmalonic acid (S- MMA)] were retrieved from the database. In this paper, we focused on tHcy and variables related to tHcy (serum folate, serum vitamin B 12 , S-MMA, plasma creatinine as well as B-Hb and B-MCV). eGFR was calculated according to the Modification of Diet in Renal Disease-4 formula (age, sex, ethnicity and plasma creatinine) [24] . Serum albumin and body mass in- dex (BMI) were used as biomarkers of general nutritional status.

Because information about the use of folate supplementation was not recorded in the database, we used 35 nmol/l as a cutoff for serum folate to discriminate between subjects with and without folic acid supplementation. Subjects with a serum folate 1 35 nmol/l were ex- cluded from all statistical analyses related to tHcy. This cutoff has been shown to discrimi- nate quite well between users and non-users of folic acid supplements [25] . In the dementia group, there were 7 subjects (1.6%) with serum folate 1 35 nmol/l and in the non-dementia group, there were 3 subjects (1.8%).

Biochemical Assays

Venous blood samples were drawn with minimal venous stasis as a part of the routine de- mentia examination program between 8: 00 and 10: 00 a.m., and the samples were immediate- ly delivered to the laboratory staff. The serum or plasma biomarker analyses were performed at the Department of Clinical Chemistry, Örebro Medical Center Hospital, Sweden, except for S-MMA which was analyzed by mass spectrometry at the Department of Clinical Chemistry, Central Hospital, Karlstad, Sweden. The local reference range of S-MMA is ! 0.37 ␮ mol/l (CV (coefficient of variance): 6.8%) and the tHcy reference range is ! 15 ␮ mol/l (CV: 4.1%).

Demented and Non-Demented Swedish Elderly

Statistical Analyses

Statistical analyses were performed using SPSS for Windows, release 16 (SPSS Inc., Chi- cago, Ill., USA). None of the continuous variables were normally distributed according to Kolmogorov-Smirnov goodness-of-fit test and thus, analyses were performed on logarithmi- cally transformed data. The descriptive results are presented as means 8 SD. Statistical sig- nificance was considered with a two-sided probability value ^ 0.05. Student’s t test was used for statistical analysis of differences between groups of continuous variables and ␹ ² tests were used for categorical variables. The patient history data were coded as binary variables (yes/

no). Associations between variables were assessed using Spearman rank correlations. Multi- variate logistic regression analyses was carried out with the forward logistic regression meth- od, with dementia/non-dementia being the dependent variable.

Ethics

The Regional Ethical Review Board, Uppsala, Sweden, approved the study.

Results

A total of 686 of the examined 926 subjects fulfilled the diagnostic criteria of dementia.

The remaining 240 were categorized as non-demented. The baseline characteristics of the subjects are shown in table 1 . The subjects in the dementia group were marginally older than subjects in the non-dementia group. Demented subjects also more frequently had a positive family history of dementia and more often received high-dose oral or intermittent paren- teral vitamin B ₁₂ prescriptions than non-demented subjects. The MMSE was significantly lower in the dementia group (p ! 0.001) than in the non-dementia group. There were no sig-

Table 1. B aseline characteristics of the 926 subjects studied

Non-dementia (n = 240)

Dementia (n = 686)

p*

Age, years 77.989.6 79.587.3 0.010

Female sex, n/total n (%) 144/240 (60.0) 416/686 (60.6) 0.163

Positive family history of dementia, n/total n (%) 52/167 (31.1) 191/481 (39.7) 0.049

B-Hb, g/l 131.7815.9 130.8815.5 0.536

MCV, fl 90.085.8 90.084.9 0.899

BMI 24.084.3 24.084.0 0.997

Serum albumin, g/l 36.884.6 36.684.6 0.565

Plasma creatinine, ␮mol/l 93.9831.6 94.1846.7 0.662

eGFR, ml/min/1.73 m² 59.3819.6 59.9818.9 0.730

Systolic BP, mm Hg 149.8825.4 149.2823.8 0.783

Diastolic BP, mm Hg 79.5812.5 78.9811.7 0.544

MMSE 23.584.9 16.386.1 <0.001

Vitamin-B12 prescription, n/total n (%) 47/240 (19.6) 213/686 (31.0) 0.001

Plasma tHcy, ␮mol/l 18.4489.4 20.689.1 0.088

S-MMA, ␮mol/l 0.2380.15 0.3280.36 0.176

D ata are means 8 SD, unless otherwise indicated. BP = Blood pressure. * Pearson ␹² or t test as ap- propriate (calculated on logarithmically transformed variables).

Demented and Non-Demented Swedish Elderly

nificant differences between dementia and non-dementia concerning B-Hb, B-MCV, BMI, serum albumin, eGFR, systolic or diastolic blood pressure.

Table 2 shows crude bivariate analysis (Spearman rank) of the associations of the select- ed biochemical parameters with age. Significant associations were seen between age and tHcy (R = 0.243; p ! 0.001), age and MMA (R = 0.550; p ! 0.001), age and B-Hb (R = –0.253;

p ! 0.001), age and serum albumin (R = –0.272; p ! 0.001), age and plasma creatinine (R = 0.164; p ! 0.001), age and eGFR (R = –0.225; p ! 0.001), and age and BMI (R = –0.159; p ! 0.001).

Table 3 shows the vitamin B 12 - and folate-related variables (e.g. tHcy, S-MMA, B-Hb and B-MCV) in relation to presence or absence of vitamin B ₁₂ prescription. In the dementia group, there were 7 subjects (1.8%) with serum folate 1 35 nmol/l and in the non-dementia group, there were 3 subjects (1.8%). These cases were all excluded from the statistical calcu-

Table 2. B ivariate association between age and selected variables from table 1

P-tHcy S-MMA Age B-Hb B-MCV S-Alb P-Crea BMI eGFR

P-tHcy Correlation coefficient Significance (two-tailed) n

1.000 257

0.471 0.001 46

0.243

<0.001 257

–0.147 0.021 249

0.011 0.878 212

–0.049 0.449 246

0.245

<0.001 247

–0.122 0.061 234

–0.259

<0.001 247 S-MMA Correlation coefficient

Significance (two-tailed) n

0.471 0.001 46

1.000 61

0.550

<0.001 61

–0.478

<0.001 60

0.092 0.515 52

–0.303 0.018 60

0.323 0.012 60

0.234 0.086 55

–0.355 0.005 60 Age Correlation coefficient

Significance (two-tailed) n

0.243

<0.001 257

0.550

<0.001 61

1.000 926

–0.253

<0.001 753

–0.060 0.162 544

–0.272

<0.001 704

0.164

<0.001 728

–0.159

<0.001 704

–0.225

<0.001 728 B-Hb Correlation coefficient

Significance (two-tailed) n

–0.147 0.021 249

–0.478

<0.001 60

–0.253

<0.001 753

1.000 753

0.062 0.151 544

0.417

<0.001 693

–0.003 0.926 714

0.223

<0.001 622

0.025 0.505 714 B-MCV Correlation coefficient

Significance (two-tailed) n

0.011 0.878 212

0.092 0.515 52

–0.060 0.162 544

0.062 0.151 544

1.000 753

0.046 0.295 522

0.048 0.272 523

0.029 0.526 491

–0.044 0.318 523 S-Alb Correlation coefficient

Significance (two-tailed) n

–0.049 0.449 246

–0.303 0.018 60

–0.272

<0.001 704

0.417

<0.001 693

0.046 0.295 522

1.000 704

0.064 0.093 687

0.163

<0.001 592

–0.043 0.259

687 P-Crea Correlation coefficient

Significance (two-tailed) n

0.245

<0.001 247

0.323 0.012 60

0.164

<0.001 728

–0.003 0.926 714

0.048 0.272 523

0.064 0.093 687

1.000 728

0.166

<0.001 610

–0.997

<0.001 728 BMI Correlation coefficient

Significance (two-tailed) n

–0.122 0.061 234

0.234 0.086 55

–0.159

<0.001 704

0.223

<0.001 622

0.029 0.526 491

0.163

<0.001 592

0.166

<0.001 610

1.000 703

–0.153

<0.001 610 eGFR Correlation coefficient

Significance (two-tailed) n

–0.259

<0.001 247

–0.355 0.005 60

–0.225

<0.001 728

0.025 0.505 714

–0.044 0.318 523

–0.043 0.259 687

–0.997

<0.001 728

–0.153

<0.001 610

1.000 728 p values according to nonparametric two-tailed Spearman correlation calculations. P-tHcy = Plasma tHcy; S-Alb = se- rum albumin; P-Crea = plasma creatinine.

Demented and Non-Demented Swedish Elderly

lations. Both dementia and non-dementia subjects with a vitamin B 12 prescription had sig- nificantly higher tHcy levels (p = 0.001 and ! 0.001, respectively) but lower serum folate (non-dementia: p ! 0.001; dementia: p = 0.006). S-MMA was also significantly higher in subjects with vitamin B ₁₂ prescription, both in the dementia and the non-dementia groups (p = 0.032 and 0.023, respectively). B-Hb was significantly lower in vitamin B 12 -prescribed dementia (p = 0.004) and non-dementia (p = 0.004) subjects than in subjects not prescribed vitamin B 12 .

Table 4 shows the tHcy-related variables in relation to family history of dementia. Among subjects with a positive family history of dementia, mean tHcy was significantly higher in demented subjects than in non-demented subjects (p = 0.021). Non-demented subjects with a positive family history of dementia had significantly higher eGFR than non-demented sub- jects without a family history of dementia (p = 0.032).

Table 5 depicts differences in biomarkers in non-demented and demented subjects ac- cording to HCS state. There were no significant differences in serum vitamin B 12 or in serum folate between the dementia and the non-dementia groups. The mean tHcy level was sig-

Table 3. B iochemical parameters according to vitamin B₁₂ prescription state and dementia diagnosis

Variable Non-dementia n p¹ Dementia n p¹ p²

S-B₁₂, pmol/l +B₁₂ –B12

292.88250.4 349.88233.2

24 100

0.020 334.08325.5 317.88168.2

126 231

0.025 0.654 0.340 S-folate, nmol/l +B12

–B₁₂

8.683.4 11.686.5

39 121

0.006 8.384.0 10.785.3

153 265

<0.001 0.454 0.351 P-tHcy, ␮mol/l +B12

–B12

22.7811.5 15.985.8

29 43

0.001 24.089.0 17.688.3

77 79

<0.001 0.267 0.389 S-MMA, ␮mol/l +B12

–B12

0.3880.21 0.1980.10

5 13

0.023 0.4680.50 0.2480.16

17 15

0.032 0.885 0.254 B-Hb, g/l +B12

–B₁₂

125.7817.6 134.3815.0

36 120

0.004 127.7814.9 132.3815.4

150 249

0.004 0.400 0.242 B-MCV, fl +B₁₂

–B12

88.086.4 90.884.9

27 92

0.015 90.884.8 89.884.8

123 186

0.099 0.011 0.137 S-Alb, g/l +B₁₂

–B12

36.185.3 37.284.5

35 117

0.167 35.484.2 36.984.4

146 242

0.001 0.534 0.537 P-Crea, ␮mol/l +B12

–B₁₂

91.2823.5 94.2834.0

38 119

0.874 89.1830.4 91.8829.2

146 248

0.274 0.458 0.668 eGFR

ml/min/1.73 m² +B₁₂ –B12

59.1815.3 59.2820.7

38 119

0.710 60.3819.7 59.6818.4

146 242

0.561 0.707 0.847

BMI +B₁₂

–B12

23.583.9 24.284.3

35 106

0.404 23.483.7 24.184.2

133 223

0.126 0.867 0.799 V alues are means 8 SD. p values are calculated by t test on logarithmically transformed variables.

S-B₁₂ = Serum vitamin B₁₂; P-tHcy = plasma tHcy; S-Alb = serum albumin; P-Crea = plasma creatinine;

+B₁₂ = has been prescribed vitamin B₁₂; –B₁₂ = has not been prescribed vitamin B₁₂. ¹ Difference between the +B₁₂ prescription and –B₁₂ prescription groups. ² Difference between the non-dementia and dementia groups.

Demented and Non-Demented Swedish Elderly

nificantly higher in the non-dementia group with HCS (p = 0.007) and borderline signifi- cantly higher in the dementia group with HCS (p = 0.064). Likewise, mean S-MMA was higher in the non-demented subgroup with HCS (p = 0.021) and tended to be higher in the demented subgroup with HCS (p = 0.140). Furthermore, there was a significant difference in eGFR between demented and non-demented subjects receiving HCS. Non-demented sub- jects with HCS had lower eGFR than demented subjects with HCS (p = 0.034). Subjects re- ceiving HCS had both significantly lower B-Hb (dementia: p ! 0.001; non-dementia: p = 0.037) and serum albumin (dementia: p ! 0.001; non-dementia: p = 0.004) compared with subjects without HCS. BMI was found to be significantly lower in subjects in the dementia group receiving HCS compared to demented subjects without HCS (p = 0.05). This difference was not seen in non-demented subjects with and without HCS.

Table 6 shows the odds ratio of having a diagnosis of dementia in relation to the three patient history variables as calculated by multivariate logistic regression analysis. Use of HCS, a family history of dementia and prescription of vitamin B 12 preparations were posi- tively associated with increased risk of dementia.

Table 4. H cy-related biomarkers in relation to family history of dementia and data completeness (t test statistics)

Variable Non-dementia n p¹ Dementia n p¹ p²

S-B12, pmol/l +FH –FH

303.88137.1 330.08247.2

31 60

0.912 272.48121.0 340.88265.0

107 147

0.136 0.253 0.917 S-folate, nmol/l +FH

–FH

12.487.7 11.385.7

36 76

0.521 10.885.7 10.185.1

120 167

0.236 0.225 0.087 P-tHcy, ␮mol/l +FH

–FH

15.183.9 18.888.9

13 35

0.168 20.689.4 20.286.9

37 59

0.744 0.021 0.191 S-MMA, ␮mol/l +FH

–FH

0.1980.13 0.2680.20

7 6

0.431 0.4880.74 0.2780.17

8 13

0.605 0.219 0.736

B-Hb, g/l +FH

–FH

133.7814.3 135.0815.6

34 75

0.615 133.1812.9 131.1815.5

114 159

0.183 0.980 0.081

B-MCV, fl +FH

–FH

90.885.9 89.885.2

27 58

0.444 89.485.1 90.684.5

87 125

0.074 0.252 0.284 S-Alb, g/l +FH

–FH

38.284.3 37.684.5

35 72

0.521 37.983.4 36.284.3

111 151

<0.001 0.842 0.024 P-Crea, ␮mol/l +FH

–FH

85.6822.7 96.0830.2

45 90

0.047 88.1824.6 95.6861.6

148 222

0.312 0.517 0.323 eGFR

ml/min/1.73 m² +FH –FH

64.0817.2 57.7819.2

45 90

0.032 61.5816.3 60.9820.3

148 222

0.277 0.425 0.323

BMI +FH

–FH

24.184.6 24.384.6

34 70

0.867 24.683.8 23.584.1

109 145

0.024 0.438 0.252 V alues are means 8 SD. p values are calculated by t test on logarithmically transformed variables.

S-B₁₂ = Serum vitamin B₁₂; P-tHcy = plasma tHcy; S-Alb = serum albumin; P-Crea = plasma creatinine;

+FH = positive family history of dementia; –FH = negative family history of dementia. ¹ Difference be- tween the +FH and –FH groups. ² Difference between the non-dementia and dementia groups.

Demented and Non-Demented Swedish Elderly

Discussion

Demented subjects more often received vitamin B 12 supplementation than did the non- demented subjects. Despite high-dose oral or intermittent parenteral vitamin B ₁₂ supple- mentation, demented subjects still had significantly higher tHcy values and lower B-Hb and serum albumin than non-supplemented demented subjects. At the same time, there were no significant differences in B-MCV, BMI or eGFR.

Table 5. B iochemical parameters according to the HCS state and dementia diagnosis

Variable Non-dementia n p¹ Dementia n p¹ p²

S-B₁₂, pmol/l +HCS –HCS

314.08177.5 353.98266.2

45 78

0.521 317.38197.7 326.98261.8

164 182

0.754 0.998 0.280 S-folate, nmol/l +HCS

–HCS

10.185.9 11.386.1

60 99

0.137 9.384.7 10.385.3

195 211

0.064 0.461 0.167 P-tHcy, ␮mol/l +HCS

–HCS

22.4812.0 16.385.6

28 44

0.007 21.487.9 20.1810.3

73 80

0.064 0.942 0.050 S-MMA, ␮mol/l +HCS

–HCS

0.4080.21 0.2080.11

4 14

0.021 0.4980.59 0.2880.18

12 20

0.140 0.929 0.090

B-Hb, g/l +HCS

–HCS

129.0817.3 134.4814.8

60 95

0.037 127.4813.8 133.5815.8

198 198

<0.001 0.602 0.624

B-MCV, fl +HCS

–HCS

90.686.0 89.985.0

45 73

0.537 90.384.8 90.184.8

147 153

0.703 0.765 0.830 S-Alb, g/l +HCS

–HCS

35.684.9 37.884.5

57 94

0.004 35.584.3 37.284.3

186 191

<0.001 0.993 0.328 P-Crea, ␮mol/l +HCS

–HCS

98.5835.2 91.3828.9

74 119

0.153 89.0826.2 99.1860.7

257 263

0.016 0.517 0.957 eGFR

ml/min/1.73 m²

+HCS –HCS

56.4820.1 60.7818.8

74 119

0.096 61.5819.1 58.5818.9

257 263

0.037 0.034 0.180

BMI +HCS

–HCS

23.584.5 24.484.1

48 92

0.180 23.484.0 24.284.0

161 185

0.050 0.988 0.791 V alues are means 8 SD. p values are calculated by t test on logarithmically transformed variables.

S-B₁₂ = Serum vitamin B₁₂; P-tHcy = plasma tHcy; S-Alb = serum albumin; P-Crea = plasma creatinine;

+HCS = has HCS; –HCS = has not HCS. ¹ Difference between the +HCS and –HCS groups. ² Difference between the non-dementia and dementia groups.

Condition (yes/no) OR for dementia (95% CI) p Prescription of vitamin B₁₂ (yes) 2.01 (1.29–3.13) 0.002 Family history of dementia (yes) 1.50 (1.02–2.19) 0.032

HCS (yes) 1.47 (1.01–2.13) 0.044

Table 6. O dds ratio for dementia associated with different

conditions

Demented and Non-Demented Swedish Elderly

Hcy is regarded as an independent risk marker of dementia and Alzheimer’s disease [10–12] . The association between vitamin B ₁₂ and folate deficiency and dementia has been observed even in subjects without hematological signs of vitamin B deficiency [26] . Unfor- tunately, tHcy concentrations in addition to vitamin B deficiency may be influenced by a large number of genetic, physiological and lifestyle factors, impaired renal function being one of the most important confounders. Proper assessment of renal function is thus crucial.

In addition to plasma creatinine, we calculated eGFR, which is considered a more precise marker of renal function.

Prior to the visit to our Memory Care Unit, clinicians had recognized the need for vita- min B ₁₂ prescriptions in a significant portion of the studied subjects. About 30% in the de- mentia group and about 20% in the non-dementia group were supplemented with vitamin B 12 at the time of the first visit at the Memory Care Unit. It is reasonable to assume that vi- tamin B ₁₂ was originally prescribed because of low serum vitamin B ₁₂ concentrations, but we were not able to retrieve data on how long the subjects had been prescribed vitamin B 12 be- fore attending the Memory Care Unit. In the present material, there were no differences in serum vitamin B 12 concentrations between subjects with or without dementia. A paradox finding was that subjects with vitamin B ₁₂ prescription actually had higher levels of both plasma tHcy and S-MMA ( table 3 ). The reason for this is obscure, but could be related to a generally inferior health status and frailty among subjects receiving vitamin B ₁₂ prescrip- tions. Those elderly receiving HCS had a poorer nutritional status and lower muscle mass.

This could result in a misinterpretation of plasma creatinine values, being lower than they should be in relation to renal function. However, renal function as judged by eGFR did not differ between the groups in our material, so this is probably not an explanation for the high- er plasma tHcy and S-MMA concentrations among patients receiving vitamin B ₁₂ supple- mentation. Other explanations could be that the prescribed vitamin B 12 doses or dosage in- tervals were insufficient to meet the demands of the patients, that bioavailability of the given vitamin B 12 preparation was too low, the duration of treatment too short, that compliance – especially in the demented group – was poor, or that many subjects suffering from vitamin B 12 deficiency simultaneously had unrecognized folate deficiency before starting with vita- min B ₁₂ supplementation. Oral vitamin B ₁₂ administration, which in Sweden nowadays is the prevailing way of supplementation [27] , has an inherent risk of poor compliance. Compared to intermittent parenteral vitamin B ₁₂ therapy, high-dose (1 mg/day) oral preparations have been demonstrated to be equally effective for maintenance therapy and even sufficient for the treatment of pernicious anemia [28] . The vitamin B 12 doses in some oral multivitamin prescription preparations might, however, have been too low to cover the needs of all patient groups [29] . At the time when the study material was collected, there was no widespread use of multivitamin prescription preparations in Sweden. In our material, we only registered high-dose oral or intermittent injectable preparations of vitamin B 12 , the by far prevailing treatment option. The notion that insufficient treatment (too low doses, too short duration, too large dosage intervals and poor compliance) might be responsible for the paradoxical finding of higher tHcy and S-MMA values among subjects on vitamin B ₁₂ treatment is cor- roborated by the observation of relatively small differences in serum vitamin B 12 concentra- tions between the supplemented and non-supplemented groups in our material (dementia:

p = 0.025; non-dementia: p = 0.020). These factors, in addition to a general poor nutritional and health status, could explain higher MMA and tHcy levels in subjects with vitamin B 12 prescriptions in our material.

HCS is obviously not a guaranty of maintaining adequate nutritional status of the en- rolled elderly subjects ( table 5 ). Under- and malnutrition is a neglected problem even among institutionalized geriatric patients in Sweden [30] . This is reflected in our material too, since tHcy was generally higher in subjects assigned to HCS. This difference was most pronounced

Demented and Non-Demented Swedish Elderly

among the non-demented subjects (p = 0.007), but we also observed a higher tHcy level in the dementia group receiving HCS, though it did not reach statistical significance (p = 0.064).

Two Finnish studies found that the majority of elderly Finnish home care patients were un- dernourished according to Mini Nutritional Assessment [31, 32] . BMI and serum albumin are useful biomarkers of the general nutritional status, especially among the elderly [33, 34] . The finding that both demented and non-demented subjects with HCS had significantly lower serum albumin than the subjects without supports the notion that HCS in our mate- rial does not provide adequate nutrition. An alternative explanation could of course be ‘con- founding-by-indication’. Indeed, BMI was also lower among patients receiving HCS, but only in the demented group (p = 0.050). The lower BMI may primarily be related to dementia itself and, as a result of this, increased requirement of HCS, rather than being caused by poorer general nutritional status as a consequence of HCS [35] . Further, HCS was a significant pre- disposing factor of dementia (odds ratio, OR 1.50, range 1.02–2.19), a finding most likely representing a reversed causality phenomenon. On the other hand, ‘meals on wheels’ com- bined with microwave heating, which is often provided by HCS, may negatively affect the vitamin B content of food [36] .

HCS is in Sweden most often provided by the local community, and most of the expen- ditures for this service are paid by taxes. This service is intended to meet the requirements of free-living elderly and to allow them to stay self-supplied as long as possible and thereby postpone premature institutionalization. Sufficient nutrition must be one of the goals of HCS. Our findings of low serum albumin, elevated Hcy, high MMA, and low serum folate indicate that there are shortcomings in the HCS with regard to provision of an adequate nu- tritional status among the elderly in the studied group. Hcy has been proposed as a suitable biomarker for malnutrition [37–39] .

We hypothesized that the group with a positive family history of dementia, which could indicate involvement of inherited factors in the development of dementia, would present changes in Hcy-related biomarkers. Indeed, we found a higher tHcy concentration in de- mented subjects with a positive family history of dementia ( table 4 ). A possible explanation might be malfunction in the folate metabolism due to genetic polymorphisms, e.g. carrier state of the common methylenetetrahydrofolate reductase (MTHFR) 677C 1 T polymor- phism [40] . Another possibility that we have looked into previously could be mutations in folate receptor- ␣ [41, 42] .

High tHcy has previously been proposed to be an independent risk factor for dementia [11, 12, 43, 44] . Our findings support a potential connection between high tHcy levels and dementia and that this association might be partly related to inherited factors and partly to environmental factors, such as poor nutrition. A positive family history of dementia in- creased the OR of having a dementia diagnosis by a factor of 1.5. This is a slightly lower OR compared to earlier epidemiological findings in a Swedish population-based sample, where the relative risk for subjects with a positive family history of dementia was 3.2 [17] .

Perhaps the most likely explanation of the higher levels of tHcy concentrations in sub- jects prescribed vitamin B ₁₂ is that supplementation with vitamin B ₁₂ may induce a relative intracellular folate deficiency due to increased intracellular demands of folate. Increase in tHcy after mono-supplementation with vitamin B ₁₂ has been reported earlier [45] . Consis- tent with this ‘folate stress’ hypothesis, both dementia and non-dementia subjects with vita- min B 12 prescription also had significantly lower serum levels of folate. However, this hy- pothesis does not explain the elevated MMA concentrations in the same patient group.

A limitation of this study is that the database does not include information about the prescription of folic acid or the duration of and compliance with vitamin B ₁₂ supplementa- tion, but we know that in 1995–2000, when the present study population was recruited, the use of multi-B vitamin prescriptions containing lower vitamin B ₁₂ doses than vitamin B ₁₂

Demented and Non-Demented Swedish Elderly

mono-tablets (0.5 vs. 1 mg/tablet) in Sweden was not widespread, and we used a serum folate cutoff level of 35 nmol/l as an exclusion criterion, which has been proposed to discriminate quite well between those taking folic acid supplements (including subjects taking over-the- counter multi-B vitamins) and those who do not [25] . Another restraint is that the data set was not complete with regard to medical history information and blood biomarkers in all subjects. While medical history information could be retrieved in almost all cases, informa- tion on biochemical parameters was in part incomplete.

In summary, we observed that tHcy levels were higher among subjects who were supple- mented with vitamin B 12 . This finding could not be explained by poorer renal function among these subjects. Further, we identified a positive family history of dementia and the need for HCS as contributing factors to this paradoxical finding. Thus, regular monitoring of the nutritional status in elderly geriatric patients is necessary. A broader approach to im- prove nutrition especially among demented elderly is warranted [46] . HCS providers might need to pay greater attention to nutrition and compliance in demented and non-demented subjects. We advocate a more active use of biomarkers as an aid to earlier identify subjects being at risk of nutritional insufficiency and to improve quality of health care among free- living as well as institutionalized elderly.

Acknowledgements

This study was supported by grants from the Örebro County Council, Örebro Univer- sity, and Nyckelfonden. We thank Dr. Lars H. Breimer for his valuable comments on the manuscript.

Disclosure Statement

None of the authors declare any conflict of interest.

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